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Therapeutic administration of a modified alpha1 proteinase inhibitor

a technology of proteinase inhibitor and therapeutic administration, which is applied in the direction of biocide, animal husbandry, peptide/protein ingredients, etc., can solve the problems of slow progress in hiv vaccines and therapy, problems with delivery and stability, and high cost of soluble cd4 as a therapeutic agen

Inactive Publication Date: 2002-01-10
BRISTOW CYNTHIA L
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  • Summary
  • Abstract
  • Description
  • Claims
  • Application Information

AI Technical Summary

Benefits of technology

0020] The method of this invention involves (a) initially confirming the existence of an {acute over (.alpha.)}.sub.1Proteinase Inhibitor deficiency in the effected population of individuals that can benefit from this type of replacement therapy, and (b) administering a therapeutic effective amount of a modified {acute over (.alpha.)}.sub.1Proteinase Inhibitor ({acute over (.alpha.)}.sub.1PI) to an individual within the effected population so as to inhibit and/or prevent {acute over (.alpha.)}.sub.1PI facilitated HIV entry into heal

Problems solved by technology

The use of soluble CD4 as a therapeutic agent is expensive, however, and there are problems with delivery and stability.
Progress in HIV vaccines and therapy has been slow due to the heterogeneous nature of the virus and the lack of suitable animal models.
While a variety of approaches have been taken to formulate pharmaceutical agents suitable for AIDS therapy, many if not all of the drugs create serious side effects which greatly limit their usefulness as therapeutic agents.
Unfortunately, inhibitors of aspartyl proteases are non-selective and therefore toxic when used in vivo.
AZT causes serious side effects, however, such that many patients cannot tolerate its administration.
Other nucleoside analogues that inhibit HIV, reverse transcriptase have been found to cause even more serious side effects then does AZT.
Unfortunately, these peptides have the side effect of mimicking the immunosuppression of HIV infection by inhibiting proliferation of T4 cells and are, thus, useless for therapy.

Method used

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Examples

Experimental program
Comparison scheme
Effect test

examples

[0028] The therapeutic method of this invention is based upon the use of a modified {acute over (.alpha.)}.sub.1PI to replace depleted circulating concentrations of endogenous {acute over (.alpha.)}.sub.1PI, while at the same time prevent {acute over (.alpha.)}.sub.1PI facilitated HIV entry. As noted briefly herein, the engineering of a modified {acute over (.alpha.)}.sub.1PI for the method of this invention is based upon the fuinctions / properties of {acute over (.alpha.)}.sub.1PI in covalent inhibition of proteinases, and the structure of the of {acute over (.alpha.)}.sub.1PI.

[0029] Properties & Structure of {acute over (.alpha.)}.sub.1PI --The amino acids involved in covalent or reversible proteinase inhibition (domain 1) lie between Glu (346) and Pro (369). The second known function of {acute over (.alpha.)}.sub.1PI involves its influence on receptor patching and cell motility. The amino acids involved in receptor patching and cell motility (domain 2) lie between Pro (369) and Pr...

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Abstract

A method for the treatment of asymtomatic HIV seropositive individuals to inhibit onset of an AIDS infection and, for suppression of propagation of HIV infections in individuals with a fully developed AIDS infection. The method consists of administering a therapeutic effective amount of a modified {acute over (alpha)}1Proteinase Inhibitor (m{acute over (alpha)}1PI) to an individual within the effected population so as to inhibit and / or prevent {acute over (alpha)} PI facilitated HIV entry into healthy / uninfected cells.

Description

[0001] This application claimsthe filing date of Provisional Patent Application No. 60 / 215,987 filed Jul. 5, 2000.[0002] 1. Field of the Invention[0003] This invention relates to a method and to a composition of matter suitable for use in this method. More specifically, this invention relates to the treatment of asymtomatic HIV seropositive individuals with a modified form of ({acute over (.alpha.)}.sub.1proteinase inhibitor (6,PI) as a means for inhibition of HIV replication in asymtomatic HIV seropositive individuals; and, as a means for suppression of propagation of HIV infections in individuals with a fully developed AIDS infection.[0004] 2. Description of the Prior Art[0005] HIV-1 is the name given to a group of highly related viruses which have been identified as the primary etiologic agent of the acquired immunodeficiency syndrome (AIDS) and AIDS related condition (ARC) in humans. HIV-1, also known as HTLV-III, LAV and ARV, is a major worldwide health problem. HIV is a relati...

Claims

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Application Information

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IPC IPC(8): A61K31/00A61K38/55
CPCA61K31/00A61K38/55
Inventor BRISTOW, CYNTHIA L.
Owner BRISTOW CYNTHIA L
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